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首页> 外文期刊>The journal of physical chemistry, B. Condensed matter, materials, surfaces, interfaces & biophysical >Long-Term-Stable Ether-Lipid vs Conventional Ester-Lipid Bicelles in Oriented Solid-State NMR: Altered Structural Information in Studies of Antimicrobial Peptides
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Long-Term-Stable Ether-Lipid vs Conventional Ester-Lipid Bicelles in Oriented Solid-State NMR: Altered Structural Information in Studies of Antimicrobial Peptides

机译:定向固态NMR中的长期稳定的醚脂与常规酯脂双细胞的关系:抗菌肽研究中改变的结构信息

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Recently, ether lipids have been introduced as long-term stable alternatives to the more natural, albeit easier degradable, ester lipids in the preparation of oriented lipid bilayers and bicelles for oriented-sample solid-state NMR spectroscopy. Here we report that ether lipids such as the frequently used 14-O-PC (1,2-di-O-tetradecyl-so-glycero-3-phosphocholine) may induce significant changes in the structure and dynamics, including altered interaction between peptides and lipids relative to what is observed with the more conventionally used DMPC (1,2-dimyristoyl-sn-gIycero-3-phosphocholine) bilayers. Such effects are demonstrated for the antimicrobial peptide novicidin, for which 2D separate-local-field NMR and circular dichroism experiments reveal significant structural/conformational differences for the peptide in the two different lipid systems. Likewise, we observe altered secondary structure and different temperature-dependent membrane anchoring for the antimicrobial peptide alamethicin depending on whether the peptide is reconstituted into ester or ether lipids. Such observations are not particularly surprising considering the significant difference of the lipids in the phosphorus headgroup and they may provide important new insight into the delicate peptide—membrane interactions in the systems studied. In contrast, these observations reinforce the need to carefully consider potential structural changes in addition to long-term stability prior to the selection of membrane environment of membrane proteins in the analysis of their structure and dynamics. In more general terms, the results underscore the necessity in structural biology to address both the protein and its environments in studies relating structure to function.
机译:最近,在制备用于定向样品固态NMR光谱的定向脂质双层和Bicells的过程中,已将醚脂质作为更稳定,更易降解的天然酯酯的长期稳定替代品。在这里,我们报道醚类脂,例如常用的14-O-PC(1,2-二-O-十四烷基-soso-glycero-3-phosphocholine)可能会诱导结构和动力学发生重大变化,包括改变肽段之间的相互作用相对于更传统使用的DMPC(1,2-二肉豆蔻酰基-sn-甘油三磷酸胆碱)双层膜观察到的脂质和脂质。对于抗菌肽新霉素,证明了这种作用,为此,二维分离局部核磁共振和圆二色性实验揭示了在两个不同脂质系统中该肽的显着结构/构象差异。同样,我们观察到抗菌肽alamethicin的二级结构发生了变化,并依赖于不同的温度依赖性膜锚定,具体取决于该肽是重构为酯还是醚脂质。考虑到磷头基团中脂质的显着差异,这些观察结果并不令人感到意外,并且它们可能为研究系统中的微妙的肽-膜相互作用提供重要的新见解。相反,这些观察结果表明,在分析膜蛋白的结构和动力学时,除了长期稳定性之前,还需要仔细考虑潜在的结构变化,以及长期稳定性。从更笼统的意义上讲,结果强调了结构生物学在研究结构与功能有关的研究中解决蛋白质及其环境的必要性。

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